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Objective: Autophagy is the regulated catabolic process for recycling damaged or unnecessary organelles, which plays crucial roles in cell survival during nutrient deficiency, and innate immune defense against pathogenic microorganisms. Autophagy has been also reported to be involved in various conditions including inflammatory diseases. IRGM (human immunity-related GTPase) has an important function in eliminating Mycobacterium tuberculosis from host cells via autophagy. We examined the association between genetic polymorphism and clinical course/outcome in severely septic patients.

Methods: The study included 125 patients with severe sepsis/septic shock (SS) and 104 non-sepsis patients who were admitted to the intensive care unit (ICU) of Chiba University Hospital between October 2001 and September 2008 (discovery cohort) and 268 SS patients and 454 non-sepsis patients who were admitted to ICUs of five Japanese institutions including Chiba University Hospital between October 2008 and September 2012 (multi-center validation cohort). Three hundred forty seven healthy volunteers who consented to this study were also included. Genotyping was performed for a single-nucleotide polymorphism (SNP) within the coding region of IRGM, IRGM(+313) (rs10065172). Lipopolysaccharide challenge of whole blood from randomly selected healthy volunteers (n = 70) was performed for comparison of IRGM mRNA expression among different genotypes.

Results: No significant difference in genotypic distributions (CC/CT/TT) at the IRGM(+313) locus was observed among the three subject groups (SS, non-sepsis, and healthy volunteers) in either cohort. When mortality were compared, no significant difference was observed in the non-sepsis group, while TT homozygotes exhibited a significantly higher mortality than the CC+CT genotype category in the SS group for both cohorts (P = 0.043, 0.037). Lipopolysaccharide challenge to whole blood showed a significant suppression of IRGM mRNA expression in TT compared with the CC+CT genotype category (P = 0.019).

Conclusions: The data suggest that the IRGM(+313), an autophagy-related polymorphic locus, influences outcome in severely septic patients, with the possible involvement of autophagy in sepsis exacerbation.

Titel:	Autophagy-related IRGM polymorphism is associated with mortality of patients with severe sepsis.
Autor/in / Beteiligte Person:	Kimura, T ; Watanabe, E ; Sakamoto, T ; Takasu, O ; Ikeda, T ; Ikeda, K ; Kotani, J ; Kitamura, N ; Sadahiro, T ; Tateishi, Y ; Shinozaki, K ; Oda, S
Link:	Volltext (PDF)
Zeitschrift:	PloS one, Jg. 9 (2014-03-13), Heft 3, S. e91522
Veröffentlichung:	San Francisco, CA : Public Library of Science, 2014
Medientyp:	academicJournal
ISSN:	1932-6203 (electronic)
DOI:	10.1371/journal.pone.0091522
Schlagwort:	Aged Cell Survival Cohort Studies Female Genotype Homozygote Humans Immunity, Innate Inflammation microbiology Japan Lipopolysaccharides chemistry Male Middle Aged Mycobacterium tuberculosis Polymorphism, Single Nucleotide Sepsis microbiology Treatment Outcome Autophagy GTP-Binding Proteins genetics Polymorphism, Genetic Sepsis genetics Sepsis mortality
Sonstiges:	Nachgewiesen in: MEDLINE Sprachen: English Publication Type: Journal Article; Research Support, Non-U.S. Gov't Language: English [PLoS One] 2014 Mar 13; Vol. 9 (3), pp. e91522. <i>Date of Electronic Publication: </i>2014 Mar 13 (<i>Print Publication: </i>2014). MeSH Terms: Autophagy* ; Polymorphism, Genetic* ; GTP-Binding Proteins / genetics ; Sepsis / genetics ; Sepsis / *mortality ; Aged ; Cell Survival ; Cohort Studies ; Female ; Genotype ; Homozygote ; Humans ; Immunity, Innate ; Inflammation / microbiology ; Japan ; Lipopolysaccharides / chemistry ; Male ; Middle Aged ; Mycobacterium tuberculosis ; Polymorphism, Single Nucleotide ; Sepsis / microbiology ; Treatment Outcome References: Nat Rev Immunol. 2013 Dec;13(12):862-74. (PMID: 24232462) ; Pediatr Clin North Am. 2008 Jun;55(3):647-68, xi. (PMID: 18501759) ; Nat Cell Biol. 2010 Dec;12(12):1154-65. (PMID: 21102437) ; Lancet. 2013 Mar 2;381(9868):774-5. (PMID: 23472921) ; Crit Care. 2013 Jul 24;17(4):R160. (PMID: 23883625) ; Immunity. 2013 Nov 14;39(5):799-800. (PMID: 24238335) ; Cell. 2004 Dec 17;119(6):753-66. (PMID: 15607973) ; Hum Mol Genet. 2010 May 1;19(9):1828-39. (PMID: 20106866) ; Nat Genet. 2007 Jul;39(7):830-2. (PMID: 17554261) ; Biometrics. 1992 Jun;48(2):361-72. (PMID: 1637966) ; Lab Invest. 2009 May;89(5):549-61. (PMID: 19188912) ; Trends Mol Med. 2009 Mar;15(3):129-38. (PMID: 19231289) ; Minerva Anestesiol. 2012 Nov;78(11):1215-25. (PMID: 22743786) ; N Engl J Med. 2003 Jan 9;348(2):138-50. (PMID: 12519925) ; Nat Genet. 2011 Mar;43(3):242-5. (PMID: 21278745) ; Nat Genet. 2007 Feb;39(2):207-11. (PMID: 17200669) ; Science. 2006 Sep 8;313(5792):1438-41. (PMID: 16888103) ; J Clin Endocrinol Metab. 2011 Apr;96(4):E633-45. (PMID: 21270330) ; Crit Care Med. 1985 Oct;13(10):818-29. (PMID: 3928249) ; N Engl J Med. 2009 Oct 15;361(16):1570-83. (PMID: 19828534) ; Am J Respir Crit Care Med. 2013 Mar 1;187(5):509-17. (PMID: 23348975) ; Infection. 2009 Jun;37(3):222-32. (PMID: 19404580) ; Crit Care Med. 1998 Nov;26(11):1793-800. (PMID: 9824069) ; Hepatology. 2011 Jun;53(6):2053-62. (PMID: 21437926) ; Ann Surg. 2011 Jun;253(6):1190-200. (PMID: 21412148) ; N Engl J Med. 2013 Feb 14;368(7):651-62. (PMID: 23406030) ; Inflamm Bowel Dis. 2009 Apr;15(4):501-7. (PMID: 18985712) ; Methods. 2001 Dec;25(4):402-8. (PMID: 11846609) ; JAMA. 2011 Dec 21;306(23):2594-605. (PMID: 22187279) ; J Exp Med. 2011 Dec 19;208(13):2581-90. (PMID: 22110166) ; Crit Care Med. 1992 Jun;20(6):864-74. (PMID: 1597042) ; Intensive Care Med. 2000 Dec;26(12):1786-93. (PMID: 11271086) ; Crit Care Med. 2006 Sep;34(9):2439-46. (PMID: 16791110) ; Crit Care Med. 1997 Aug;25(8):1298-307. (PMID: 9267941) ; Am J Respir Crit Care Med. 2010 Sep 15;182(6):745-51. (PMID: 20538956) Substance Nomenclature: 0 (Lipopolysaccharides) ; EC 3.6.1.- (GTP-Binding Proteins) ; EC 3.6.1.- (IRGM protein, human) Entry Date(s): Date Created: 20140315 Date Completed: 20160129 Latest Revision: 20211021 Update Code: 20231215 PubMed Central ID: PMC3953488

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Autophagy-related IRGM polymorphism is associated with mortality of patients with severe sepsis.